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#' Obtain LOH data
#'
#' Obtain LOH heatmap on entire chromsomes from samples in a cohort
#' @name lohSpec_slidingWindow
#' @param loh_data data frame with columns "chromosome", "position", "n_vaf",
#' "t_vaf", "sample" giving raw vaf calls for germline variants
#' @param step integer with the length of divisions (bp) in chromosomes
#' @param window_size integer with the size of the sliding window (bp) to be
#' applied
#' @param normal integer specifying the normal VAF frequency used in LOH
#' calculations
#' @return object of class dataframe containing LOH data
#' @importFrom plyr adply
#' @importFrom plyr ldply
#' @noRd
lohSpec_slidingWindow <- function(loh_data, step, window_size, normal)
{
## Obtain lists for each sample and chromosome
out <- split(loh_data, list(as.character(loh_data$chromosome),
as.character(loh_data$sample)))
## Obtain the window position values
window_data <- lohSpec_windowPosition(out, step, window_size)
total <- data.frame()
final_dataset <- list()
final_df <- list()
loh_df <- list()
## Perform loh Calculations on each chromosome and sample within each window
for (i in 1:length(out))
{
final_dataset[[i]] <- lohSpec_lohCalc(window_data[[i]], out[[i]],
normal)
#final_dataset[[i]] <- plyr::ldply(final_df[[i]], data.frame)
}
## Calculate avg loh for overlapping regions
df <- lohSpec_stepCalc(final_dataset, step = step)
## Combine the lists into a single dataframe
loh_dataset <- plyr::ldply(df, data.frame)
colnames(loh_dataset) <- c("window_start", "window_stop", "chromosome",
"sample", "loh_diff_avg")
loh_dataset$loh_diff_avg <- loh_dataset$loh_diff_avg
return(loh_dataset)
}
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